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1 lso prepared using the same DNA amplified by multiple displacement amplification.
2 other amplification methodologies including multiple displacement amplification.
3 capsulated into droplets and amplified using multiple displacement amplification.
5 s et al. present a method combining improved multiple displacement amplification and FACS, to obtain
6 using a #10 K file and then amplified using multiple displacement amplification and PCR-amplified wi
7 e-flow-sorted cells, amplifying their DNA by multiple displacement amplification and sequencing all c
8 it-depletion with phi29 DNA polymerase-based multiple displacement amplification and shotgun DNA sequ
9 he polar bodies and oocytes are amplified by multiple displacement amplification and, together with m
10 ing whole-genomic DNA prior to SNP analysis, multiple displacement amplification, and OmniPlex techno
11 e-genome amplification (SWGA), an isothermal multiple-displacement amplification-based method, to eff
12 DNA template in each aliquot is amplified by multiple displacement amplification, converted into barc
14 human donor were subjected to droplet-based multiple displacement amplification (dMDA) to generate l
16 n-sensitive restriction enzyme digestion and multiple displacement amplification for selective detect
20 (IMS) for targeted bacterial enrichment with multiple displacement amplification (MDA) for whole-geno
21 (IMS) for targeted bacterial enrichment with multiple displacement amplification (MDA) for whole-geno
24 needs to be amplified before sequencing and multiple displacement amplification (MDA) is widely used
28 form was used to generate genomic DNA by the multiple displacement amplification (MDA) technique from
31 escence-activated cell sorting, whole-genome multiple displacement amplification (MDA), and subsequen
33 first time a recently developed WGA method, multiple displacement amplification (MDA), to amplify si
37 sted the two most commonly used WGA methods, multiple displacement amplification (MDA-Qiagen REPLI-g
40 flow-sorting of single nuclei, time-limited multiple-displacement amplification (MDA), low-input lib
41 Here we present WGA-X, a method based on multiple displacement amplification of DNA that utilizes
42 MIP-Seq), an experimental approach involving multiple displacement amplification of individual provir
46 essed these issues by developing single-cell multiple displacement amplification (SCMDA) and a genera
48 st time coupled a microfluidic platform with multiple displacement amplification technology to perfor
50 have developed a method based on isothermic multiple-displacement amplification to allow access to a
51 e is exhaustive single-cell sequencing using multiple displacement amplification, which is simply int